Biology Year 11 · Module 2

The Mammalian Digestive System — Physical and Chemical Digestion

You're about to meet a patient whose digestive system isn't working. Understanding why will teach you exactly how a healthy one does.

Learning Intentions

Trace the full pathway of food from mouth to large intestine
Distinguish physical digestion from chemical digestion
Name the enzymes, substrates, and products at each digestive region
Explain how pH conditions are matched to enzyme function
Apply enzyme-substrate specificity to digestion

Outcome Links

Trace the digestion of foods in a mammalian digestive system
Describe physical digestion and chemical digestion
Relate organ system structure to heterotroph nutrient requirements (L06)
Apply hierarchical organisation — organ system level (L04)

Success Criteria

List the organs in order and state one function each
Correctly match each enzyme to its substrate, product, and location
Explain why stomach enzymes would be inactivated in the mouth
Distinguish physical and chemical digestion with examples
Write a Band 6 response on digestion of a named macromolecule

HSC Exam Relevance

Content from this lesson that appears directly in HSC Biology exams

High Priority

Enzymes — substrate, product, location, pH

Matching digestive enzymes to their substrates and products is tested in almost every HSC paper — Section I (1–2 marks) and Section II (3–4 marks). Must know salivary amylase, pepsin, pancreatic lipase, and intestinal enzymes including their pH optima.

High Priority

Physical vs chemical digestion — with examples

Distinguishing the two types of digestion and providing examples of each at specific locations appears as a 2–3 mark short answer question. Bile emulsification is the most commonly tested physical digestion example after chewing.

Medium Priority

pH and enzyme function

Explaining why different digestive regions have different pH environments and how this matches enzyme optima is tested as a 2–3 mark application question — often with a graph of enzyme activity vs pH.

Medium Priority

Tracing digestion of a specific food

"Trace the digestion of a protein-containing meal from ingestion to absorption-ready products" — this exact question type appears in HSC Section II for 4–5 marks. This lesson provides the framework; L12 covers absorption.

The Case

Patient Case — Something Is Wrong

Read the file. Then work out which part of the system has failed.

Before we look at how a healthy digestive system works, meet a patient whose doesn't. Your job as you read this lesson is to figure out — using the biology you're learning — exactly what has gone wrong and why her symptoms make perfect sense once you understand the system.

Patient File — Gastroenterology Referral

Patient

Female, 19 years

Referring Physician

GP — Central Sydney Clinic

Presenting Symptoms

Patient presents with an 8-month history of chronic fatigue, unexplained weight loss despite adequate dietary intake, abdominal bloating, and iron-deficiency anaemia unresponsive to oral iron supplements. Patient reports symptoms worsen significantly after consuming bread, pasta, and wheat-containing foods.

Investigative Findings

Blood panel: low haemoglobin, low serum ferritin, low vitamin B12, low calcium. Small intestine biopsy via endoscopy: severe villous atrophy — intestinal villi are flattened and significantly reduced in height. Positive for anti-tissue transglutaminase antibodies.

Provisional Diagnosis

Coeliac disease — autoimmune response to gluten damages intestinal villi

Your investigation: This patient eats enough food. Her digestive system breaks food down physically and chemically. But she is still severely malnourished. As you work through this lesson, identify at exactly which stage the system fails — and explain why flattened villi cause every symptom listed above. The answer is in Lesson 12 (Absorption), but the biology you need to understand it is right here.

The Central Clue

Digestion and absorption are two different processes. This patient's digestion — the breakdown of food into small molecules — is working perfectly. Something that happens after digestion is broken. Keep this in mind as you learn the digestive pathway below.

Core Content

Two Types of Digestion

Different processes, same goal — making molecules small enough to absorb

All digestion serves one purpose: converting large insoluble food molecules into small soluble molecules that can cross the intestinal wall into the bloodstream. Two fundamentally different mechanisms achieve this.

⚙ Physical Digestion

⚗ Chemical Digestion

What it does: Breaks food into smaller pieces — but does NOT change the chemical structure of molecules. A large starch molecule is still starch after chewing; it is just in smaller pieces.

What it does: Breaks chemical bonds within molecules using enzymes, converting large molecules into their monomer subunits. Starch → glucose; protein → amino acids; fat → fatty acids + glycerol.

How: Mechanical force — teeth grinding and cutting, stomach churning (peristalsis), bile breaking fat globules into droplets (emulsification)

How: Enzyme-catalysed hydrolysis — water molecules are added across chemical bonds, splitting large polymers into monomers

Why it matters: Increases surface area for chemical digestion. A 1cm cube of food has 6cm² of surface area. Cut it into 8 equal pieces and you have 12cm² — double. More surface = faster enzyme action.

Why it matters: Only small soluble monomers (glucose, amino acids, fatty acids) can be absorbed across the intestinal wall into blood. Physical digestion alone cannot produce absorbable products.

Examples: Chewing (mastication) in mouth · Stomach churning · Bile emulsification of fats in small intestine

Examples: Salivary amylase (mouth) · Pepsin (stomach) · Pancreatic lipase (small intestine) · Maltase, sucrase, lactase (small intestine)

Exam Technique

When asked to distinguish physical and chemical digestion, always include: (1) whether chemical bonds are broken, (2) a specific example with location, and (3) what is produced. A common HSC error is calling bile "chemical digestion" — bile emulsification is physical digestion because it breaks fat globules into droplets without breaking any chemical bonds in the fat molecules themselves.

The Digestive Pathway — Mouth to Large Intestine

What happens at each stop — physical processes, enzymes, pH, products

Food travels through a continuous tube approximately 9 metres long. Each region is structurally and chemically specialised for a specific stage of processing. The key is that pH, enzyme type, and mechanical action are precisely matched at every point.

🦷

Mouth

Food enters and is processed by both physical and chemical means simultaneously. Teeth cut and grind food (mastication) — physical digestion. Saliva is secreted by three pairs of salivary glands; it moistens food, lubricates swallowing, and delivers the first digestive enzyme.

Salivary amylase Substrate: starch Product: maltose

pH ≈ 6.5–7.0 · Enzyme optimum: neutral/slightly acidic

↕️

Oesophagus

A muscular tube connecting the mouth to the stomach. No digestion occurs here — the oesophagus is purely a transport structure. Rhythmic waves of muscular contraction called peristalsis push the food bolus downward. The cardiac sphincter at the base prevents stomach acid from refluxing upward.

No enzymes · Peristalsis only

🔴

Stomach

The stomach is a muscular bag that performs vigorous churning — a powerful form of physical digestion that converts the food bolus into a semi-liquid paste called chyme. Simultaneously, gastric glands in the stomach lining secrete hydrochloric acid (HCl) and the enzyme pepsinogen.

HCl does two things: it kills most bacteria in food, and it converts inactive pepsinogen into active pepsin. Pepsin only works in strongly acidic conditions — this is why the stomach maintains a dramatically low pH.

Pepsin Substrate: proteins Product: polypeptides (partial) HCl secreted

pH ≈ 1.5–3.5 · Strongly acidic · Pepsin optimum: pH 2

🟢

Small Intestine — the Main Digestion and Absorption Chamber

The small intestine is where the vast majority of chemical digestion is completed and where essentially all nutrient absorption occurs. It has three regions: duodenum (receives secretions from pancreas and liver), jejunum (primary absorption zone), and ileum (continued absorption, vitamin B12).

When acidic chyme enters the duodenum, the pancreas secretes sodium bicarbonate to neutralise it — raising pH to around 7–8 and creating conditions suitable for pancreatic enzymes. The liver produces bile, stored in the gall bladder and released into the duodenum; bile salts emulsify fat globules into tiny droplets, dramatically increasing surface area for lipase action.

Pancreatic amylase Starch → maltose

Pancreatic lipase Triglycerides → fatty acids + glycerol

Trypsin + chymotrypsin Polypeptides → shorter peptides

Maltase · Sucrase · Lactase Disaccharides → monosaccharides (glucose etc.)

Peptidases Peptides → amino acids

pH ≈ 7.0–8.5 · Alkaline (neutralised by NaHCO₃ from pancreas)

🟡

Large Intestine (Colon)

By the time material reaches the large intestine, chemical digestion is essentially complete. The large intestine's primary role is water and electrolyte reabsorption — converting the liquid contents into solid faeces. Resident bacteria ferment undigested material (mainly dietary fibre), producing some vitamins (K, B12) as byproducts that are absorbed here.

No digestive enzymes secreted · Water reabsorption · Bacterial fermentation · Faeces formation

pH Across the System

Notice the dramatic pH change from stomach (pH ~2) to small intestine (pH ~7.5). This is not accidental — it is precisely regulated. Pepsin is denatured above pH 4, so it automatically becomes inactive when chyme is neutralised in the duodenum. Pancreatic enzymes have optima around pH 7–8, which is exactly the environment the bicarbonate creates. Each region's pH is perfectly matched to activate its own enzymes and inactivate those from the previous region.

Enzyme-Substrate Specificity

Why amylase digests starch but not protein — and why this matters clinically

Each digestive enzyme has an active site with a shape complementary to one specific substrate — the lock-and-key (or induced-fit) model. This specificity is not a limitation; it is a feature. It means the digestive system can process proteins, carbohydrates, and fats simultaneously without interference, and it means each enzyme only acts on its intended substrate.

✗ Common Misconceptions

✓ What's Actually True

"Amylase digests all carbohydrates"

Amylase only breaks α-1,4 glycosidic bonds in starch and glycogen. It cannot digest cellulose (β-1,4 bonds) — which is why dietary fibre passes through undigested.

"Pepsin works throughout the digestive system"

Pepsin is irreversibly denatured above pH 4. It only functions in the stomach. When chyme enters the duodenum and is neutralised, pepsin is immediately inactivated — protein digestion is then continued by trypsin and chymotrypsin.

"Bile is a digestive enzyme"

Bile contains bile salts — detergent-like molecules that emulsify fats physically. No chemical bonds are broken. Bile is a physical digestion agent, not an enzyme.

"Lactose intolerance means you can't digest dairy"

Lactase deficiency means the enzyme lactase is absent or reduced. Lactose (milk sugar) reaches the large intestine undigested, where bacteria ferment it — causing gas, bloating, and discomfort. All other dairy nutrients (protein, fat) are digested normally.

Back to the Patient

Notice that our patient's enzyme system is working perfectly — all four enzyme types are present, pH conditions are correct, physical digestion is normal. Starch, protein, and fat are all being broken down to their absorbable monomers. Yet she is malnourished. This confirms that the failure is not in digestion — it is in what happens to the products of digestion. That's Lesson 12.

Complete Enzyme Reference

Everything you need to know — one reference card

Use this card to check your recall. Cover the right-hand columns and test yourself on each enzyme before the assessment.

Enzyme	Source	Location active	Substrate	Product	pH optimum
Salivary amylase	Salivary glands	Mouth	Starch	Maltose	~7.0
Pepsin	Gastric glands (as pepsinogen, activated by HCl)	Stomach	Proteins	Polypeptides	~2.0
Pancreatic amylase	Pancreas	Small intestine (duodenum)	Starch / remaining polysaccharides	Maltose	~7.0
Pancreatic lipase	Pancreas	Small intestine (duodenum)	Triglycerides (after bile emulsification)	Fatty acids + glycerol	~7.5
Trypsin / chymotrypsin	Pancreas	Small intestine	Polypeptides	Shorter peptides	~8.0
Maltase	Small intestine epithelium	Small intestine	Maltose	Glucose + glucose	~7.0
Sucrase	Small intestine epithelium	Small intestine	Sucrose	Glucose + fructose	~7.0
Lactase	Small intestine epithelium	Small intestine	Lactose	Glucose + galactose	~6.0
Peptidases	Small intestine epithelium	Small intestine	Dipeptides / short peptides	Amino acids	~7.5

Pattern to Remember

Carbohydrate digestion starts in the mouth and finishes in the small intestine. Protein digestion starts in the stomach and finishes in the small intestine. Fat digestion only occurs in the small intestine (bile emulsification is needed first). All three nutrient types produce absorbable monomers by the end of the small intestine — which is where Lesson 12 picks up.

Copy into your books

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Physical vs Chemical Digestion

Physical: breaks food into smaller pieces — NO bond breaking. Examples: chewing, churning, bile emulsification.
Chemical: breaks bonds using enzymes (hydrolysis). Examples: amylase, pepsin, lipase.
Bile = physical digestion (emulsification only — not an enzyme).

Key Enzyme Facts

Salivary amylase: mouth, starch → maltose, pH 7.
Pepsin: stomach, protein → polypeptides, pH 2.
Pancreatic lipase: small intestine, triglycerides → fatty acids + glycerol.
Maltase/sucrase/lactase: small intestine, disaccharides → monosaccharides.

pH Across Regions

Mouth: pH ~7 (neutral — amylase active).
Stomach: pH ~2 (acidic — pepsin active; HCl secreted).
Small intestine: pH ~7.5 (alkaline — pancreatic NaHCO₃ neutralises chyme).
Pepsin denatures above pH 4 — automatically inactivated in duodenum.

Digestion Start Points

Carbohydrates: mouth (amylase) → small intestine (completed).
Proteins: stomach (pepsin) → small intestine (completed).
Fats: small intestine only (bile emulsification then lipase).
All three produce absorbable monomers in the small intestine.

Activities

Activity 01

Investigating the Patient — Connecting Symptoms to Biology

Use what you've learned in this lesson to begin explaining the patient's symptoms.

Return to the patient file at the start of this lesson. For each symptom below, use your knowledge of the digestive system to suggest which biological process you would expect to be affected. (You won't be able to explain the mechanism fully until L12 — but you should be able to identify where in the system the problem lies.)

The patient eats adequate iron in her diet but has iron-deficiency anaemia and does not respond to oral iron supplements. What does this tell you about her digestive process vs her absorption process?
The patient's biopsy shows "villous atrophy" — flattened villi. Based on what you know about the small intestine's role, predict what general consequence villous atrophy would have on nutrient availability.
The patient's symptoms worsen after eating wheat products (bread, pasta). Wheat contains gluten — a protein. Which enzyme(s) would digest gluten, and in which organ(s)?
Her symptoms include weight loss despite eating enough food. Using the distinction between digestion and absorption, explain how this is possible.

Type here or answer in your book. Full answers revealed after L12.

Activity 02

Tracing a Meal — Physical and Chemical Digestion

A classic HSC question type — trace the digestion of a specific food from ingestion to absorbable products.

A student eats a ham and cheese sandwich with a glass of milk. The sandwich contains: bread (starch), ham (protein), cheese (protein and fat), and milk (lactose, protein, fat). For each macromolecule, trace its complete digestion from the mouth to the point where it becomes absorbable, naming: the physical digestion steps, the enzyme(s) involved, the location(s), and the final absorbable products.

Cover three macromolecules: starch (from bread), protein (from ham/cheese/milk), and fat (from cheese/milk). Include lactose separately.

Activity 03

pH and Enzyme Function — Graph Interpretation

Interpreting enzyme activity vs pH graphs is a core HSC working scientifically skill.

The following data shows the activity of three digestive enzymes at different pH values.

pH	Salivary amylase activity (%)	Pepsin activity (%)	Pancreatic lipase activity (%)
1	5	90	0
2	10	100	0
4	40	60	5
6	85	10	30
7	100	2	70
8	60	0	100
9	20	0	65
10	5	0	20

Identify the pH optimum of each enzyme and explain why this matches the pH of the region where each enzyme is active.
Explain what happens to pepsin activity when chyme moves from the stomach into the duodenum (pH rises from ~2 to ~7.5). Refer to enzyme structure in your answer.
A patient takes antacid medication that raises stomach pH to approximately 5. Predict and explain the effect on protein digestion.
Salivary amylase continues acting on starch in the stomach for a short time after swallowing. Using the data, explain at what point salivary amylase activity would cease, and why.

Type here or answer in your book.

Assessment

Multiple Choice

Select the best answer — feedback shown immediately

1. Bile is produced by the liver and released into the duodenum. Which of the following correctly classifies bile's role in digestion?

Chemical digestion — bile contains lipase enzymes that break down triglycerides into fatty acids and glycerol.

Chemical digestion — bile breaks chemical bonds in fat molecules, converting them into absorbable monomers.

Physical digestion — bile salts emulsify large fat globules into small droplets, increasing surface area for lipase without breaking any chemical bonds in the fat.

Physical digestion — bile neutralises stomach acid in the duodenum, creating optimal conditions for fat digestion.

2. A person with a deficiency in pancreatic lipase would experience difficulty digesting which macromolecule, and where would the problem first become apparent?

Fats — in the small intestine, where pancreatic lipase is the primary enzyme responsible for fat digestion.

Proteins — in the stomach, where pepsin normally begins protein digestion.

Carbohydrates — in the mouth, where amylase would fail to initiate starch digestion.

Fats — in the stomach, where gastric lipase would no longer be supplemented by pancreatic enzymes.

3. Pepsinogen is secreted in an inactive form and requires HCl to become active pepsin. Which of the following best explains the biological advantage of this arrangement?

It prevents pepsin from digesting food in the oesophagus during swallowing.

It allows the liver to control the rate of protein digestion by regulating HCl production.

It allows salivary amylase to finish carbohydrate digestion before protein digestion begins.

It prevents active pepsin from digesting the protein-containing cells of the gastric glands that produce it — protecting the stomach lining.

4. A student claims that physical digestion is unnecessary — the enzymes could break down food even without mechanical processing. Which statement best evaluates this claim?

The claim is correct — enzymes can digest any size of food molecule as long as they are present in sufficient concentration.

The claim is incorrect — physical digestion increases the surface area of food available for enzyme action; without it, enzyme digestion would be far slower as enzymes can only act on exposed surfaces.

The claim is partially correct — physical digestion is needed only for proteins, as carbohydrates and fats can dissolve without mechanical processing.

The claim is incorrect — physical digestion produces the absorbable monomers; enzymes only assist in transport across the intestinal wall.

5. Which sequence correctly traces the chemical digestion of a starch molecule from ingestion to its final absorbable product?

Starch → glucose (mouth, salivary amylase) → absorbed in stomach

Starch → maltose (stomach, pepsin) → glucose (small intestine, amylase)

Starch → maltose (mouth + small intestine, amylase) → glucose + glucose (small intestine, maltase)

Starch → polypeptides (small intestine, amylase) → glucose (large intestine, bacterial enzymes)

Short Answer

6. Trace the complete digestion of a protein from ingestion to absorbable products. In your answer, name the enzymes involved, state where each acts, identify the pH conditions, and state the final products. 5 MARKS

Five points: mouth (none), stomach (pepsin + pH), small intestine (trypsin/chymotrypsin + peptidases), final product.

7. Explain why the stomach must maintain a strongly acidic pH (approximately 2) and why this pH would be harmful in the small intestine. 3 MARKS

8. Distinguish between physical digestion and chemical digestion. In your answer, provide one example of each from different regions of the digestive system, and explain how physical digestion supports chemical digestion. 4 MARKS

Comprehensive Answers

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Multiple Choice

1. C — Bile emulsification is physical digestion. Bile salts are detergent-like molecules that break large fat globules into tiny droplets, increasing surface area for lipase action. No chemical bonds in fat molecules are broken by bile. Bile does not contain lipase (that is the pancreas) and its neutralising effect is from bicarbonate ions, not bile salts.

2. A — Pancreatic lipase is the primary fat-digesting enzyme in the small intestine. Fat digestion only begins in the small intestine (after bile emulsification), so a lipase deficiency would manifest there. Fats would pass through undigested, causing fatty stools (steatorrhoea).

3. D — Pepsinogen is secreted inactive to protect the gastric gland cells from self-digestion. The cells themselves are made of protein — if active pepsin were secreted directly, it could digest the cells that produce it. Activation only occurs in the stomach lumen (away from the cell) when HCl is present.

4. B — Physical digestion increases surface area, which directly increases the rate of enzyme action. Enzymes can only act on substrate molecules they can access — an intact large food piece has a small surface area relative to its mass. Cutting it into smaller pieces exposes far more surface for simultaneous enzyme contact.

5. C — Starch → maltose by salivary amylase (mouth) then pancreatic amylase (small intestine) → glucose + glucose by maltase (small intestine). Pepsin does not act on starch; amylase does not produce glucose directly; large intestine does not complete starch digestion.

Q6 — Model Answer

In the mouth, protein is physically broken into smaller pieces by mastication (chewing) to increase surface area. No chemical digestion of protein occurs in the mouth — salivary amylase only acts on starch.

In the stomach (pH ~1.5–3.5), gastric glands secrete pepsinogen and hydrochloric acid (HCl). HCl activates pepsinogen to pepsin. Pepsin is a protease with an optimum pH of ~2 — it cleaves peptide bonds within protein chains, producing shorter polypeptides.

In the small intestine (pH ~7.5 — neutralised by NaHCO₃ from the pancreas), the pancreas secretes trypsin and chymotrypsin, which continue cleaving polypeptides into shorter peptide fragments. Pepsin is denatured at this pH and ceases to function.

Peptidases on the brush border of the intestinal epithelium cleave the remaining peptide bonds, producing individual amino acids — the final absorbable products.

Q7 — Model Answer

The stomach must maintain pH ~2 for two reasons: first, this activates pepsinogen to active pepsin (pepsin has an optimum pH of ~2 and is only functional in strongly acidic conditions); second, the acidic environment kills most bacteria and pathogens present in ingested food.

A pH of 2 in the small intestine would be harmful because pancreatic enzymes (amylase, lipase, trypsin, chymotrypsin) have pH optima around 7–8 and would be denatured or strongly inhibited at pH 2. This would prevent digestion of carbohydrates, fats, and proteins in the small intestine. To prevent this, the pancreas secretes sodium bicarbonate into the duodenum, which neutralises the acidic chyme and raises pH to approximately 7.5 before pancreatic enzymes act.

Q8 — Model Answer

Physical digestion breaks food into smaller pieces without altering the chemical structure of the molecules — no bonds are broken and no new products are formed. An example is bile emulsification in the small intestine: bile salts break large fat globules into tiny droplets, increasing the surface area of fat available for enzyme action, but the triglyceride molecules themselves are chemically unchanged.

Chemical digestion breaks covalent bonds within food molecules using enzymes via hydrolysis reactions, converting large insoluble polymers into small soluble monomers. An example is pepsin acting on proteins in the stomach (pH ~2): pepsin cleaves peptide bonds within protein chains, converting proteins into shorter polypeptides.

Physical digestion supports chemical digestion by increasing the surface area of food available for enzyme contact. Since enzyme reactions occur at the surface of substrate molecules, a smaller particle size means more substrate surface is simultaneously accessible — dramatically increasing the rate of chemical digestion. Without physical digestion, enzyme action would be limited to the outer surface of large food pieces, significantly slowing the overall process.

Mark lesson as complete

The patient mystery resolves in Lesson 12 — tick when you're ready.

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